Low-dose Lidocaine Suppresses Experimentally Induced Hyperalgesia in Humans 

医学 麻醉 利多卡因 伤害 局部麻醉剂 痛觉过敏 伤害感受器 有害刺激 组胺 丸(消化) 补品(生理学) 静脉局部麻醉 止痛药 痛阈 药理学 外科 内科学 受体
作者
Wolfgang Koppert,Susanne Zeck,Reinhard Sittl,Rudolf Likar,Ralph Knöll,Martin Schmelz
出处
期刊:Anesthesiology [Lippincott Williams & Wilkins]
卷期号:89 (6): 1345-1353 被引量:114
标识
DOI:10.1097/00000542-199812000-00011
摘要

Background The antinociceptive effects of systemically administered local anesthetics have been shown in various conditions, such as neuralgia, polyneuropathy, fibromyalgia, and postoperative pain. The objective of the study was to identify the peripheral mechanisms of action of low-dose local anesthetics in a model of experimental pain. Methods In a first experimental trial, participants (n=12) received lidocaine systemically (a bolus injection of 2 mg/kg in 10 min followed by an intravenous infusion of 2 mg x kg(-1) x h(-1) for another 50 min). In a second trial, modified intravenous regional anesthesia was administered to exclude possible central analgesic effects. In one arm, patients received an infusion of 40 ml lidocaine, 0.05%; in their other arm, 40 ml NaCl, 0.9%, served as a control. In both trials, calibrated tonic and phasic mechanical and chemical (histamine) stimuli were applied to determine differentially the impairment of tactile and nociceptive perception. Results Mechanical sensitivity to touch, phasic mechanical stimuli of noxious intensity, and heat pain thresholds remained unchanged after systemic and regional application of the anesthetic. In contrast, histamine-induced itch (intravenous regional anesthesia), axon reflex flare (systemic treatment), and development of acute mechanical hyperalgesia during tonic pressure (12 N; 2 min) of an interdigital web was significantly suppressed after both treatments. Conclusions Increasing painfulness during sustained pinching has been attributed to excitation and simultaneous sensitization of particular Adelta- and C-nociceptors. This hyperalgesic mechanism seems to be particularly sensitive to low concentrations of lidocaine. These findings confirm clinical experience with lidocaine in pain states dominated by hyperalgesia.
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